首页> 外文期刊>Biomacromolecules >Single-Site Cys-Substituting Mutation of Human Lectin Galectin-2: Modulating Solubility in Recombinant Production, Reducing Long-Term Aggregation, and Enabling Site-Specific MonoPEGylation
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Single-Site Cys-Substituting Mutation of Human Lectin Galectin-2: Modulating Solubility in Recombinant Production, Reducing Long-Term Aggregation, and Enabling Site-Specific MonoPEGylation

机译:人凝集素galectin-2的单站点Cys替代突变:调节重组生产中的溶解度,减少长期聚集,并实现位点特异性单聚乙二醇化。

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摘要

The effector capacity of endogenous lectins on cell adhesion/growth prompts studies to turn them into pharmaceutically stable forms. Using human galectin-2 as a proof-of-principle model, we first introduced mutations at the site of one of the two Cys residues, that is, C57A, C57M, and C57S. Only the C57M variant was expressed in bacteria in soluble form in high yield. No notable aggregation of the modified homodimeric lectin occurred during 3 weeks of storage. This mutational process also facilitated the site-directed introduction of poly(ethylene glycol) into the remaining sulfhydryl group (Cys75). Product analysis revealed rather complete conjugation with one chain per subunit in the homodimer. We note that neither the secondary structure alteration nor the absence of binding ability to a glycoprotein (asialofetuin) was observed. The results thus document the feasibility of tailoring a human galectin for enhanced stability to aggregation as well as monoPEGylation, which enables further testing of biological properties including functionality as growth regulator and the rate of serum clearance.
机译:内源性凝集素对细胞粘附/生长的效应能力促使研究将其转变为药物稳定形式。我们使用人galectin-2作为原理证明模型,首先在两个Cys残基之一C57A,C57M和C57S的位点处引入了突变。仅C57M变体以可溶形式在细菌中以高产率表达。在储存3周期间没有发生修饰的同二聚凝集素的明显聚集。此突变过程还有助于将聚乙二醇定向引入剩余的巯基(Cys75)。产物分析显示在同型二聚体中每个亚基具有一个完整的缀合。我们注意到,既没有观察到二级结构改变,也没有观察到对糖蛋白(asialofetuin)的结合能力。因此,结果证明了定制人半乳凝素以增强聚集稳定性和单聚乙二醇化的可行性,这使得能够进一步测试生物学特性,包括作为生长调节剂的功能和血清清除率。

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